Literature DB >> 23821544

The Legionella pneumophila GTPase activating protein LepB accelerates Rab1 deactivation by a non-canonical hydrolytic mechanism.

Ashwini K Mishra1, Claudia M Del Campo, Robert E Collins, Craig R Roy, David G Lambright.   

Abstract

GTPase activating proteins (GAPs) from pathogenic bacteria and eukaryotic host organisms deactivate Rab GTPases by supplying catalytic arginine and glutamine fingers in trans and utilizing the cis-glutamine in the DXXGQ motif of the GTPase for binding rather than catalysis. Here, we report the transition state mimetic structure of the Legionella pneumophila GAP LepB in complex with Rab1 and describe a comprehensive structure-based mutational analysis of potential catalytic and recognition determinants. The results demonstrate that LepB does not simply mimic other GAPs but instead deploys an expected arginine finger in conjunction with a novel glutamic acid finger, which forms a salt bridge with an indispensible switch II arginine that effectively locks the cis-glutamine in the DXXGQ motif of Rab1 in a catalytically competent though unprecedented transition state configuration. Surprisingly, a heretofore universal transition state interaction with the cis-glutamine is supplanted by an elaborate polar network involving critical P-loop and switch I serines. LepB further employs an unusual tandem domain architecture to clamp a switch I tyrosine in an open conformation that facilitates access of the arginine finger to the hydrolytic site. Intriguingly, the critical P-loop serine corresponds to an oncogenic substitution in Ras and replaces a conserved glycine essential for the canonical transition state stereochemistry. In addition to expanding GTP hydrolytic paradigms, these observations reveal the unconventional dual finger and non-canonical catalytic network mechanisms of Rab GAPs as necessary alternative solutions to a major impediment imposed by substitution of the conserved P-loop glycine.

Entities:  

Keywords:  GAP; GTPase; GTPase Activating Protein; Host-Pathogen Interactions; Legionella pneumophila; LepB; Rab; Rab Proteins; Rab1; X-ray Crystallography

Mesh:

Substances:

Year:  2013        PMID: 23821544      PMCID: PMC3745345          DOI: 10.1074/jbc.M113.470625

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  50 in total

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  13 in total

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Review 8.  Rab GTPases and their interacting protein partners: Structural insights into Rab functional diversity.

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9.  Mutant enzymes challenge all assumptions.

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10.  Yersinia pestis Requires Host Rab1b for Survival in Macrophages.

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